in this double-blind trial patients were randomized to optimal therapy with captopril (4909), valsartan (4909) in dosages up to 160 mg bid, or a combination of the two drugs (4885) within ten days of myocardial infarction complicated by left ventricular dysfunction or heart failure. Approximately 70% of patients were on beta blockers
in order to be included patients had to have clinical/ECG evidence and biomarker evidence of an acute myocardial infarct within the previous 10 days
also there was a requirement for clinical or radiological evidence of heart failure and/or left ventricular dysfunction (LVD) on the echocardiogram
clinical signs used to indicate heart failure were bilateral post-tussive rales in at least the lower third of lung fields or an S3 gallop with persistent tachycardia
patients were randomised into one of three groups
valsartan treatment alone (target dose 160mg twice a day), or,
captopril treatment alone (target dose 50mg three times a day), or,
a combination of captopril and valsartan (target doses 50mg three times a day and 80mg twice daily respectively)
doses were titrated up in four steps
primary endpoint was all-cause mortality. The secondary endpoint was cardiovascular-related morbidity and mortality
there was no difference in mortality rates, which were approximately 20% for all three treatment groups
the rate of rehospitalization for myocardial infarction and heart failure approached 20% for all three groups
the valsartan-and-captopril group had the most drug-related adverse events
with monotherapy, hypotension and renal dysfunction were more common in the valsartan group, and cough, rash, and taste disturbance were more common in the captopril group
the study authors concluded that Valsartan is as effective as captopril in patients who are at high risk for cardiovascular events after myocardial infarction. Also combining valsartan with captopril increased the rate of adverse events without improving survival.This study also demonstrated that valsartan treatment resulted in a significantly lower level of treatment discontinuations due to adverse drug events in comparison to captopril treatment (1,2)
a subsequent study (3) concluded that:
angiotensin receptor blockers appear to be as effective as ACE inhibitors in reducing atherosclerotic events, even when used in addition to other secondary preventive treatments
these data, although not conclusive, also support the hypothesis that adding an ARB to an ACE inhibitor may have a small additional anti-infarction effect, a possibility that needs to be prospectively tested
Add information to this page that would be handy to have on hand during a consultation, such as a web address or phone number. This information will always be displayed when you visit this page